Clinical pharmacokinetics of quetiapine:
an atypical antipsychotic
by
DeVane CL, Nemeroff CB.
Department of Psychiatry and Behavioral Sciences,
Medical University of South Carolina,
Charleston 29425, USA.
devanel@musc.edu
Clin Pharmacokinet 2001;40(7):509-22
ABSTRACT
Quetiapine is a dibenzothiazepine derivative that
has been evaluated for management of patients with the manifestations of
psychotic disorders. In pharmacokinetic studies in humans, quetiapine was
rapidly absorbed after oral administration, with median time to reach maximum
observed plasma concentration ranging from 1 to 2 hours. The absolute bioavailability
is unknown, but the relative bioavailability from orally administered tablets
compared with a solution was nearly complete. Food has minimal effects on
quetiapine absorption. The drug is approximately 83% bound to serum proteins.
Single and multiple dose studies have demonstrated linear pharmacokinetics
in the clinical dose range (up to 375mg twice daily). The drug is eliminated
with a mean terminal half-life of approximately 7 hours. The primary route
of elimination is through hepatic metabolism. In vitro studies show that
quetiapine is predominantly metabolised by cytochrome P450 (CYP) 3A4. After
administration of [14C]quetiapine, approximately 73% of the radioactivity
was excreted in the urine and 21% in faeces. Quetiapine accounted for less
than 1% of the excreted radioactivity. 11 metabolites formed through hepatic
oxidation have been identified. Two were found to be pharmacologically active,
but they circulate in plasma at 2 to 12% of the concentration of quetiapine
and are unlikely to contribute substantially to the pharmacological effects
of the drug. The pharmacokinetics of quetiapine do not appear to be altered
by cigarette smoking. Oral clearance declines with age, and was reduced
in 2 of 8 patients with hepatic dysfunction but not in patients with renal
impairment. Quetiapine has no effect on the in vitro activity of CYP1A2,
2C9, 2C19, 2D6 and 3A4 at clinically relevant concentrations. The lack of
effect of quetiapine on hepatic oxidation was confirmed in vivo by the lack
of effect of quetiapine on antipyrine disposition. Quetiapine had no effect
on serum lithium concentration. Phenytoin and thioridazine increase the
clearance of quetiapine, and ketoconazole decreases clearance. No clinically
significant effects of cimetidine, haloperidol, risperidone or imipramine
on the pharmacokinetics of quetiapine were noted. Quetiapine dosage adjustment,
therefore, may be necessary when coadministered with phenytoin, thioridazine
or other potent CYP3A4 inducers or inhibitors. The relationship between
the therapeutic effects and the plasma concentrations of quetiapine has
been investigated in a multicentre clinical trial. There was no statistically
significant association between trough plasma quetiapine concentration and
clinical response as measured by traditional assessments of psychotic symptom
severity. Subsequent clinical studies of the plasma concentration versus
effect relationships for quetiapine may help to further define guidelines
for dosage regimen design.
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